Literature DB >> 15937278

DOM-fold: a structure with crossing loops found in DmpA, ornithine acetyltransferase, and molybdenum cofactor-binding domain.

Hua Cheng1, Nick V Grishin.   

Abstract

Understanding relationships between sequence, structure, and evolution is important for functional characterization of proteins. Here, we define a novel DOM-fold as a consensus structure of the domains in DmpA (L-aminopeptidase D-Ala-esterase/amidase), OAT (ornithine acetyltransferase), and MocoBD (molybdenum cofactor-binding domain), and discuss possible evolutionary scenarios of its origin. As shown by a comprehensive structure similarity search, DOM-fold distinguished by a two-layered beta/alpha architecture of a particular topology with unusual crossing loops is unique to those three protein families. DmpA and OAT are evolutionarily related as indicated by their sequence, structural, and functional similarities. Structural similarity between the DmpA/OAT superfamily and the MocoBD domains has not been reported before. Contrary to previous reports, we conclude that functional similarities between DmpA/OAT proteins and N-terminal nucleophile (Ntn) hydrolases are convergent and are unlikely to be inherited from a common ancestor.

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Year:  2005        PMID: 15937278      PMCID: PMC2253344          DOI: 10.1110/ps.051364905

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


  45 in total

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  11 in total

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7.  Autoproteolytic activation of ThnT results in structural reorganization necessary for substrate binding and catalysis.

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Review 8.  Divergence and convergence in enzyme evolution.

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9.  MALISAM: a database of structurally analogous motifs in proteins.

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10.  Exploring the role of conformational heterogeneity in cis-autoproteolytic activation of ThnT.

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